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3 results

  • Topical tamoxifen in the therapy of cutaneous leishmaniasis

  • CRISTIANA T. TRINCONI, JULIANA Q. REIMÃO, VIVIAN I. BONANO, CAROLINE R. ESPADA, DANILO C. MIGUEL, JENICER K. U. YOKOYAMA-YASUNAKA, SILVIA R. B. ULIANA
  • Journal:
    Parasitology / Volume 145 / Issue 4 / April 2018
    Published online by Cambridge University Press:
    09 March 2017, pp. 490-496
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  • The aims of the present work were to test the effect of tamoxifen administered topically and the therapeutic efficacy of tamoxifen and pentavalent antimonial combinations in an experimental model of cutaneous leishmaniasis. BALB/c mice infected with a luciferase expressing line of Leishmania amazonensis were treated with topical tamoxifen in two different formulations (ethanol or oil-free cream) as monotherapy or in co-administration with pentavalent antimonial. Treatment efficacy was evaluated by lesion size and parasite burden, quantified through luminescence, at the end of treatment and 4 weeks later. Topical tamoxifen, formulated in ethanol or as a cream, was shown to be effective. The interaction between tamoxifen and pentavalent antimonial was additive in vitro. Treatment with combined schemes containing tamoxifen and pentavalent antimonial was effective in reducing lesion size and parasite burden. Co-administration of tamoxifen and pentavalent antimonial was superior to monotherapy with antimonial.

  • Development and Evaluation of a Novel Topical Treatment for Acne with Azelaic Acid-Loaded Nanoparticles

  • Catarina Pinto Reis, Ana Gomes, Patrícia Rijo, Sara Candeias, Pedro Pinto, Marina Baptista, Nuno Martinho, Lia Ascensão
  • Journal:
    Microscopy and Microanalysis / Volume 19 / Issue 5 / October 2013
    Published online by Cambridge University Press:
    15 May 2013, pp. 1141-1150
    Print publication:
    October 2013

  • Azelaic acid (AzA) is used in the treatment of acne. However, side effects and low compliance have been associated with several topical treatments with AzA. Nanotechnology presents a strategy that can overcome these problems. Polymeric nanoparticles can control drug release and targeting and reduce local drug toxicity. The aim of this study was to produce and evaluate an innovative topical treatment for acne with AzA-loaded poly-dl-lactide/glycolide copolymer nanoparticles. A soft white powder of nanoparticles was prepared. The mean size of loaded nanoparticles was <400 nm and zeta potential was negative. Spherical nanoparticles were observed by scanning electron microscopy. Encapsulation efficiency was around 80% and a strong interaction between the polymer and the drug was confirmed by differential scanning calorimetric analysis. In vitro drug release studies suggested a controlled and pulsatile release profile. System efficacy tests suggested similar results between the loaded nanoparticles and the nonencapsulated drug against the most common bacteria associated with acne. Cytotoxicity of AzA-loaded nanoparticles was concentration dependent, although not pronounced. The occluded patch test seemed to indicate that the formulation excipients were safe and thus AzA-loaded nanoparticles appear to be an efficient and safe treatment for acne.

  • Endoscopic management of rhinocerebral mucormycosis with topical and intravenous amphotericin B

  • B Saedi, M Sadeghi, P Seilani
  • Journal:
    The Journal of Laryngology & Otology / Volume 125 / Issue 8 / August 2011
    Published online by Cambridge University Press:
    10 June 2011, pp. 807-810
    Print publication:
    August 2011
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  • Objective:

    Mucormycosis is an aggressive fungal infection which may still cause fatal complications. However, the rarity of this disease has made optimal treatment a controversial issue. This study aimed to evaluate the use of topical amphotericin B in endoscopic management of rhinocerebral mucormycosis.

    Subjects and methods:

    Thirty patients with infection limited to the nose and sinuses were selected. Patients underwent endoscopic debridement of all necrotic tissue; cottonoid pledgets soaked in amphotericin B solution were then placed in the nasal cavity. Subsequently, long-term antifungal therapy was administered.

    Results:

    The overall survival rate was 60 per cent (18 cases); survival rates in the diabetic and malignancy groups were 70.58 and 40 per cent, respectively. Apart from predisposing factors, orbital and maxillary sinus involvement also had a significant correlation with patient outcome.

    Conclusion:

    Topical use of amphotericin B combined with endoscopic surgical debridement, followed by intravenous amphotericin B treatment, may constitute acceptable management for selected patients, with less morbidity than conventional treatments.